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多巴胺D2受体介导的对嗅神经末梢的突触前抑制。

Dopamine D2 receptor-mediated presynaptic inhibition of olfactory nerve terminals.

作者信息

Ennis M, Zhou F M, Ciombor K J, Aroniadou-Anderjaska V, Hayar A, Borrelli E, Zimmer L A, Margolis F, Shipley M T

机构信息

Department of Anatomy and Neurobiology and Program in Neuroscience, University of Maryland School of Medicine, Baltimore, Maryland 21201, USA.

出版信息

J Neurophysiol. 2001 Dec;86(6):2986-97. doi: 10.1152/jn.2001.86.6.2986.

Abstract

Olfactory receptor neurons of the nasal epithelium project via the olfactory nerve (ON) to the glomeruli of the main olfactory bulb, where they form glutamatergic synapses with the apical dendrites of mitral and tufted cells, the output cells of the olfactory bulb, and with juxtaglomerular interneurons. The glomerular layer contains one of the largest population of dopamine (DA) neurons in the brain, and DA in the olfactory bulb is found exclusively in juxtaglomerular neurons. D2 receptors, the predominant DA receptor subtype in the olfactory bulb, are found in the ON and glomerular layers, and are present on ON terminals. In the present study, field potential and single-unit recordings, as well as whole cell patch-clamp techniques, were used to investigate the role of DA and D2 receptors in glomerular synaptic processing in rat and mouse olfactory bulb slices. DA and D2 receptor agonists reduced ON-evoked synaptic responses in mitral/tufted and juxtaglomerular cells. Spontaneous and ON-evoked spiking of mitral cells was also reduced by DA and D2 agonists, and enhanced by D2 antagonists. DA did not produce measurable postsynaptic changes in juxtaglomerular cells, nor did it alter their responses to mitral/tufted cell inputs. DA also reduced 1) paired-pulse depression of ON-evoked synaptic responses in mitral/tufted and juxtaglomerular cells and 2) the amplitude and frequency of spontaneous, but not miniature, excitatory postsynaptic currents in juxtaglomerular cells. Taken together, these findings are consistent with the hypothesis that activation of D2 receptors presynaptically inhibits ON terminals. DA and D2 agonists had no effect in D2 receptor knockout mice, suggesting that D2 receptors are the only type of DA receptors that affect signal transmission from the ON to the rodent olfactory bulb.

摘要

鼻上皮的嗅觉受体神经元通过嗅神经投射至主嗅球的小球,在那里它们与嗅球的输出细胞——二尖瓣细胞和簇状细胞的顶端树突以及近小球间神经元形成谷氨酸能突触。小球层包含大脑中多巴胺(DA)神经元数量最多的群体之一,并且嗅球中的DA仅存在于近小球神经元中。D2受体是嗅球中主要的DA受体亚型,存在于嗅神经和小球层,并且位于嗅神经终末上。在本研究中,使用场电位和单单位记录以及全细胞膜片钳技术来研究DA和D2受体在大鼠和小鼠嗅球切片的小球突触处理中的作用。DA和D2受体激动剂降低了二尖瓣/簇状细胞和近小球细胞中嗅神经诱发的突触反应。DA和D2激动剂也降低了二尖瓣细胞的自发和嗅神经诱发的放电,并被D2拮抗剂增强。DA在近小球细胞中未产生可测量的突触后变化,也未改变它们对二尖瓣/簇状细胞输入的反应。DA还降低了:1)二尖瓣/簇状细胞和近小球细胞中嗅神经诱发的突触反应的双脉冲抑制;2)近小球细胞中自发但非微小兴奋性突触后电流的幅度和频率。综上所述,这些发现与D2受体在突触前抑制嗅神经终末的假说一致。DA和D2激动剂在D2受体基因敲除小鼠中没有作用,表明D2受体是影响从嗅神经到啮齿动物嗅球信号传递的唯一类型的DA受体。

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